Your search keyword '"Chuanjuan Tao"' showing total 20 results

1. Discovery of SARS-CoV-2 antiviral synergy between remdesivir and approved drugs in human lung cells

Author

Xammy Nguyenla, Eddie Wehri, Erik Van Dis, Scott B. Biering, Livia H. Yamashiro, Chi Zhu, Julien Stroumza, Claire Dugast-Darzacq, Thomas G. W. Graham, Xuanting Wang, Steffen Jockusch, Chuanjuan Tao, Minchen Chien, Wei Xie, Dinshaw J. Patel, Cindy Meyer, Aitor Garzia, Thomas Tuschl, James J. Russo, Jingyue Ju, Anders M. Näär, Sarah Stanley, and Julia Schaletzky

Subjects

Medicine, Science

Abstract

Abstract SARS coronavirus 2 (SARS-CoV-2) has caused an ongoing global pandemic with significant mortality and morbidity. At this time, the only FDA-approved therapeutic for COVID-19 is remdesivir, a broad-spectrum antiviral nucleoside analog. Efficacy is only moderate, and improved treatment strategies are urgently needed. To accomplish this goal, we devised a strategy to identify compounds that act synergistically with remdesivir in preventing SARS-CoV-2 replication. We conducted combinatorial high-throughput screening in the presence of submaximal remdesivir concentrations, using a human lung epithelial cell line infected with a clinical isolate of SARS-CoV-2. This identified 20 approved drugs that act synergistically with remdesivir, many with favorable pharmacokinetic and safety profiles. Strongest effects were observed with established antivirals, Hepatitis C virus nonstructural protein 5A (HCV NS5A) inhibitors velpatasvir and elbasvir. Combination with their partner drugs sofosbuvir and grazoprevir further increased efficacy, increasing remdesivir’s apparent potency > 25-fold. We report that HCV NS5A inhibitors act on the SARS-CoV-2 exonuclease proofreader, providing a possible explanation for the synergy observed with nucleoside analog remdesivir. FDA-approved Hepatitis C therapeutics Epclusa® (velpatasvir/sofosbuvir) and Zepatier® (elbasvir/grazoprevir) could be further optimized to achieve potency and pharmacokinetic properties that support clinical evaluation in combination with remdesivir.

Published

2022

2. Combination of antiviral drugs inhibits SARS-CoV-2 polymerase and exonuclease and demonstrates COVID-19 therapeutic potential in viral cell culture

Author

Xuanting Wang, Carolina Q. Sacramento, Steffen Jockusch, Otávio Augusto Chaves, Chuanjuan Tao, Natalia Fintelman-Rodrigues, Minchen Chien, Jairo R. Temerozo, Xiaoxu Li, Shiv Kumar, Wei Xie, Dinshaw J. Patel, Cindy Meyer, Aitor Garzia, Thomas Tuschl, Patrícia T. Bozza, James J. Russo, Thiago Moreno L. Souza, and Jingyue Ju

Subjects

Biology (General), QH301-705.5

Abstract

In this paper, the hepatitis C virus inhibitors Pibrentasvir and Ombitasvir are found to inhibit the SARS-CoV-2 exonuclease and are shown to have therapeutic potential when combined with SARS-CoV-2 polymerase inhibitors in viral cell cultures.

Published

2022

3. Identifying Structural Features of Nucleotide Analogues to Overcome SARS-CoV-2 Exonuclease Activity

Author

Xuanting Wang, Chuanjuan Tao, Irina Morozova, Sergey Kalachikov, Xiaoxu Li, Shiv Kumar, James J. Russo, and Jingyue Ju

Subjects

SARS-CoV-2, coronaviruses, antivirals, RNA-dependent RNA polymerase, exonuclease, nucleotide analogues, Microbiology, QR1-502

Abstract

With the recent global spread of new SARS-CoV-2 variants, there remains an urgent need to develop effective and variant-resistant oral drugs. Recently, we reported in vitro results validating the use of combination drugs targeting both the SARS-CoV-2 RNA-dependent RNA polymerase (RdRp) and proofreading exonuclease (ExoN) as potential COVID-19 therapeutics. For the nucleotide analogues to be efficient SARS-CoV-2 inhibitors, two properties are required: efficient incorporation by RdRp and substantial resistance to excision by ExoN. Here, we have selected and evaluated nucleotide analogues with a variety of structural features for resistance to ExoN removal when they are attached at the 3′ RNA terminus. We found that dideoxynucleotides and other nucleotides lacking both 2′- and 3′-OH groups were most resistant to ExoN excision, whereas those possessing both 2′- and 3′-OH groups were efficiently removed. We also found that the 3′-OH group in the nucleotide analogues was more critical than the 2′-OH for excision by ExoN. Since the functionally important sequences in Nsp14/10 are highly conserved among all SARS-CoV-2 variants, these identified structural features of nucleotide analogues offer invaluable insights for designing effective RdRp inhibitors that can be simultaneously efficiently incorporated by the RdRp and substantially resist ExoN excision. Such newly developed RdRp terminators would be good candidates to evaluate their ability to inhibit SARS-CoV-2 in cell culture and animal models, perhaps combined with additional exonuclease inhibitors to increase their overall effectiveness.

Published

2022

4. Nucleotide analogues as inhibitors of SARS‐CoV Polymerase

Author

Jingyue Ju, Xiaoxu Li, Shiv Kumar, Steffen Jockusch, Minchen Chien, Chuanjuan Tao, Irina Morozova, Sergey Kalachikov, Robert N. Kirchdoerfer, and James J. Russo

Subjects

COVID‐19, SARS‐CoV, SARS‐CoV‐2, RNA‐dependent RNA polymerase, nucleotide analogue, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract SARS‐CoV‐2, a member of the coronavirus family, has caused a global public health emergency. Based on our analysis of hepatitis C virus and coronavirus replication, and the molecular structures and activities of viral inhibitors, we previously reasoned that the FDA‐approved hepatitis C drug EPCLUSA (Sofosbuvir/Velpatasvir) should inhibit coronaviruses, including SARS‐CoV‐2. Here, using model polymerase extension experiments, we demonstrate that the active triphosphate form of Sofosbuvir is incorporated by low‐fidelity polymerases and SARS‐CoV RNA‐dependent RNA polymerase (RdRp), and blocks further incorporation by these polymerases; the active triphosphate form of Sofosbuvir is not incorporated by a host‐like high‐fidelity DNA polymerase. Using the same molecular insight, we selected 3’‐fluoro‐3’‐deoxythymidine triphosphate and 3’‐azido‐3’‐deoxythymidine triphosphate, which are the active forms of two other anti‐viral agents, Alovudine and AZT (an FDA‐approved HIV/AIDS drug) for evaluation as inhibitors of SARS‐CoV RdRp. We demonstrate the ability of two of these HIV reverse transcriptase inhibitors to be incorporated by SARS‐CoV RdRp where they also terminate further polymerase extension. Given the 98% amino acid similarity of the SARS‐CoV and SARS‐CoV‐2 RdRps, we expect these nucleotide analogues would also inhibit the SARS‐CoV‐2 polymerase. These results offer guidance to further modify these nucleotide analogues to generate more potent broad‐spectrum anti‐coronavirus agents.

Published

2020

5. In vitro antiviral activity of the anti-HCV drugs daclatasvir and sofosbuvir against SARS-CoV-2, the aetiological agent of COVID-19

Author

Camila R. R. Pão, Thomas Tuschl, Aitor Garzia, Lucas Villas Bôas Hoelz, Felipe Betoni Saraiva, Suelen da Silva Gomes Dias, Dumith Chequer Bou-Habib, Frederico Silva Castelo Branco, Wei Xie, Jingyue Ju, Chuanjuan Tao, Vinicius Cardoso Soares, André C. Ferreira, Stevens K. Rehen, Jairo R. Temerozo, Caroline S. de Freitas, Carine dos Santos da Silva, Carolina Q. Sacramento, Marília Zaluar P. Guimarães, Andrew Owen, Thiago Moreno L. Souza, Patrícia T. Bozza, Xuanting Wang, Nubia Boechat, Mayara Mattos, Rajith K. R. Rajoli, Dinshaw J. Patel, Steffen Jockusch, Marcelo Alves Ferreira, Fernando A. Bozza, Natalia Fintelman-Rodrigues, Gabriela Vitória, Livia Goto-Silva, Tácio Vinício Amorim Fernandes, Aline de Paula Dias Da Silva, Mônica M. Bastos, Carolina da S. G. Pedrosa, Leticia R. Q. Souza, James J. Russo, and Minchen Chien

Subjects

0301 basic medicine, Microbiology (medical), Pyrrolidines, Daclatasvir, Sofosbuvir, viruses, Biology, Pharmacology, Antiviral Agents, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, RNA polymerase, Chlorocebus aethiops, medicine, AcademicSubjects/MED00740, Animals, Humans, Pharmacology (medical), 030212 general & internal medicine, NS5A, Vero Cells, NS5B, Original Research, SARS-CoV-2, Imidazoles, COVID-19, virus diseases, RNA, Valine, biochemical phenomena, metabolism, and nutrition, In vitro, AcademicSubjects/MED00290, 030104 developmental biology, Infectious Diseases, Pharmaceutical Preparations, chemistry, Vero cell, RNA, Viral, Carbamates, AcademicSubjects/MED00230, medicine.drug

Abstract

Background Current approaches of drug repurposing against COVID-19 have not proven overwhelmingly successful and the SARS-CoV-2 pandemic continues to cause major global mortality. SARS-CoV-2 nsp12, its RNA polymerase, shares homology in the nucleotide uptake channel with the HCV orthologue enzyme NS5B. Besides, HCV enzyme NS5A has pleiotropic activities, such as RNA binding, that are shared with various SARS-CoV-2 proteins. Thus, anti-HCV NS5B and NS5A inhibitors, like sofosbuvir and daclatasvir, respectively, could be endowed with anti-SARS-CoV-2 activity. Methods SARS-CoV-2-infected Vero cells, HuH-7 cells, Calu-3 cells, neural stem cells and monocytes were used to investigate the effects of daclatasvir and sofosbuvir. In silico and cell-free based assays were performed with SARS-CoV-2 RNA and nsp12 to better comprehend the mechanism of inhibition of the investigated compounds. A physiologically based pharmacokinetic model was generated to estimate daclatasvir’s dose and schedule to maximize the probability of success for COVID-19. Results Daclatasvir inhibited SARS-CoV-2 replication in Vero, HuH-7 and Calu-3 cells, with potencies of 0.8, 0.6 and 1.1 μM, respectively. Although less potent than daclatasvir, sofosbuvir alone and combined with daclatasvir inhibited replication in Calu-3 cells. Sofosbuvir and daclatasvir prevented virus-induced neuronal apoptosis and release of cytokine storm-related inflammatory mediators, respectively. Sofosbuvir inhibited RNA synthesis by chain termination and daclatasvir targeted the folding of secondary RNA structures in the SARS-CoV-2 genome. Concentrations required for partial daclatasvir in vitro activity are achieved in plasma at Cmax after administration of the approved dose to humans. Conclusions Daclatasvir, alone or in combination with sofosbuvir, at higher doses than used against HCV, may be further fostered as an anti-COVID-19 therapy.

Published

2021

6. Sofosbuvir terminated RNA is more resistant to SARS-CoV-2 proofreader than RNA terminated by Remdesivir

Author

Chuanjuan Tao, Xiaoxu Li, Steffen Jockusch, Irina Morozova, Shiv Kumar, Minchen Chien, Sergey Kalachikov, James J. Russo, and Jingyue Ju

Subjects

0301 basic medicine, Exonucleases, Sofosbuvir, viruses, lcsh:Medicine, Hepacivirus, Viral Nonstructural Proteins, medicine.disease_cause, Virus Replication, Biochemistry, chemistry.chemical_compound, Drug Discovery, Prodrugs, lcsh:Science, Polymerase, Coronavirus, Multidisciplinary, Alanine, Coronavirus RNA-Dependent RNA Polymerase, biology, Hepatitis C, Chemical biology, RNA, Viral, Coronavirus Infections, medicine.drug, Exonuclease, Daclatasvir, Hepatitis C virus, 030106 microbiology, Pneumonia, Viral, RNA-dependent RNA polymerase, Antiviral Agents, Article, 03 medical and health sciences, Betacoronavirus, medicine, Genetics, Humans, Pandemics, SARS-CoV-2, lcsh:R, Drug Repositioning, RNA, COVID-19, medicine.disease, RNA-Dependent RNA Polymerase, Virology, Adenosine Monophosphate, 030104 developmental biology, Viral replication, chemistry, biology.protein, lcsh:Q, DNA

Abstract

SARS-CoV-2 is responsible for COVID-19, resulting in the largest pandemic in over a hundred years. After examining the molecular structures and activities of hepatitis C viral inhibitors and comparing hepatitis C virus and coronavirus replication, we previously postulated that the FDA-approved hepatitis C drug EPCLUSA (Sofosbuvir/Velpatasvir) might inhibit SARS-CoV-2.1 We subsequently demonstrated that Sofosbuvir triphosphate is incorporated by the relatively low fidelity SARS-CoV and SARS-CoV-2 RNA-dependent RNA polymerases (RdRps), serving as an immediate polymerase reaction terminator, but not by a host-like high fidelity DNA polymerase.2,3 Other investigators have since demonstrated the ability of Sofosbuvir to inhibit SARS-CoV-2 replication in lung and brain cells;4,5 additionally, COVID-19 clinical trials with EPCLUSA6 and with Sofosbuvir plus Daclatasvir7 have been initiated in several countries. SARS-CoV-2 has an exonuclease-based proofreader to maintain the viral genome integrity.8 Any effective antiviral targeting the SARS-CoV-2 RdRp must display a certain level of resistance to this proofreading activity. We report here that Sofosbuvir terminated RNA resists removal by the exonuclease to a substantially higher extent than RNA terminated by Remdesivir, another drug being used as a COVID-19 therapeutic. These results offer a molecular basis supporting the current use of Sofosbuvir in combination with other drugs in COVID-19 clinical trials.

Published

2020

7. Nucleotide Analogues as Inhibitors of SARS-CoV-2 Polymerase, a Key Drug Target for COVID-19

Author

Xiaoxu Li, Steffen Jockusch, Chuanjuan Tao, Jingyue Ju, Robert N. Kirchdoerfer, James J. Russo, Minchen Chien, Shiv Kumar, and Thomas K. Anderson

Subjects

0301 basic medicine, viruses, Hepatitis C virus, RNA-dependent RNA polymerase, medicine.disease_cause, Biochemistry, Tenofovir alafenamide, Article, 03 medical and health sciences, chemistry.chemical_compound, RNA polymerase, medicine, Polymerase, Coronavirus, Alovudine, 030102 biochemistry & molecular biology, biology, SARS-CoV-2, COVID-19, virus diseases, General Chemistry, Virology, 030104 developmental biology, chemistry, Viral replication, biology.protein, nucleotide analogues

Abstract

SARS-CoV-2 is responsible for the current COVID-19 pandemic. On the basis of our analysis of hepatitis C virus and coronavirus replication, and the molecular structures and activities of viral inhibitors, we previously demonstrated that three nucleotide analogues (the triphosphates of Sofosbuvir, Alovudine, and AZT) inhibit the SARS-CoV RNA-dependent RNA polymerase (RdRp). We also demonstrated that a library of additional nucleotide analogues terminate RNA synthesis catalyzed by the SARS-CoV-2 RdRp, a well-established drug target for COVID-19. Here, we used polymerase extension experiments to demonstrate that the active triphosphate form of Sofosbuvir (an FDA-approved hepatitis C drug) is incorporated by SARS-CoV-2 RdRp and blocks further incorporation. Using the molecular insight gained from the previous studies, we selected the active triphosphate forms of six other antiviral agents, Alovudine, Tenofovir alafenamide, AZT, Abacavir, Lamivudine, and Emtricitabine, for evaluation as inhibitors of the SARS-CoV-2 RdRp and demonstrated the ability of these viral polymerase inhibitors to be incorporated by SARS-CoV-2 RdRp, where they terminate further polymerase extension with varying efficiency. These results provide a molecular basis for inhibition of the SARS-CoV-2 RdRp by these nucleotide analogues. If sufficient efficacy of some of these FDA-approved drugs in inhibiting viral replication in cell culture is established, they may be explored as potential COVID-19 therapeutics.

Published

2020

8. Combination of Antiviral Drugs to Inhibit SARS-CoV-2 Polymerase and Exonuclease as Potential COVID-19 Therapeutics

Author

Natalia Fintelman Rodrigues, James J. Russo, Carolina Q. Sacramento, Xuanting Wang, Jingyue Ju, Aitor Garzia, Li Xaioxu, Chuanjuan Tao, Jairo R. Temerozo, Cindy Meyer, Shiv Kumar, Minchen Chien, Patrícia T. Bozza, Steffen Jockusch, Thiago Moreno L. Souza, Thomas Tuschi, Otavio Augusto Chaves, Dinshaw J. Patel, and Wei Xie

Subjects

Exonuclease, Exonucleases, Pyrrolidines, Proline, Hepatitis C virus, viruses, Favipiravir, Viral Nonstructural Proteins, medicine.disease_cause, Virus Replication, Antiviral Agents, Article, chemistry.chemical_compound, RNA polymerase, Cell Line, Tumor, Chlorocebus aethiops, medicine, Animals, Humans, Anilides, Amino Acid Sequence, NS5A, Vero Cells, Polymerase, biology, Base Sequence, Chemistry, SARS-CoV-2, RNA, COVID-19, Drug Synergism, Valine, RNA-Dependent RNA Polymerase, Virology, Pibrentasvir, COVID-19 Drug Treatment, biology.protein, RNA, Viral, Benzimidazoles

Abstract

SARS-CoV-2 has an exonuclease-based proofreader, which removes nucleotide inhibitors such as Remdesivir that are incorporated into the viral RNA during replication, reducing the efficacy of these drugs for treating COVID-19. Combinations of inhibitors of both the viral RNA-dependent RNA polymerase and the exonuclease could overcome this deficiency. Here we report the identification of hepatitis C virus NS5A inhibitors Pibrentasvir and Ombitasvir as SARS-CoV-2 exonuclease inhibitors. In the presence of Pibrentasvir, RNAs terminated with the active forms of the prodrugs Sofosbuvir, Remdesivir, Favipiravir, Molnupiravir and AT-527 were largely protected from excision by the exonuclease, while in the absence of Pibrentasvir, there was rapid excision. Due to its unique structure, Tenofovir-terminated RNA was highly resistant to exonuclease excision even in the absence of Pibrentasvir. Viral cell culture studies also demonstrate significant synergy using this combination strategy. This study supports the use of combination drugs that inhibit both the SARS-CoV-2 polymerase and exonuclease for effective COVID-19 treatment.

Published

2021

9. A Library of Nucleotide Analogues Terminate RNA Synthesis Catalyzed by Polymerases of Coronaviruses Causing SARS and COVID-19

Author

James J. Russo, Thomas K. Anderson, Shiv Kumar, Minchen Chien, Jingyue Ju, Chuanjuan Tao, Robert N. Kirchdoerfer, Xiaoxu Li, and Steffen Jockusch

Subjects

chemistry.chemical_classification, Exonuclease, biology, Base pair, viruses, virus diseases, medicine.disease_cause, Virology, Tenofovir alafenamide, chemistry.chemical_compound, chemistry, RNA polymerase, biology.protein, Nucleoside triphosphate, medicine, Nucleotide, Polymerase, Coronavirus

Abstract

SARS-CoV-2, a member of the coronavirus family, is responsible for the current COVID-19 worldwide pandemic. We previously demonstrated that five nucleotide analogues inhibit the SARS-CoV-2 RNA-dependent RNA polymerase (RdRp), including the active triphosphate forms of Sofosbuvir, Alovudine, Zidovudine, Tenofovir alafenamide and Emtricitabine. We report here the evaluation of a library of additional nucleoside triphosphate analogues with a variety of structural and chemical features as inhibitors of the RdRps of SARS-CoV and SARS-CoV-2. These features include modifications on the sugar (2’ or 3’ modifications, carbocyclic, acyclic, or dideoxynucleotides) or on the base. The goal is to identify nucleotide analogues that not only terminate RNA synthesis catalyzed by these coronavirus RdRps, but also have the potential to resist the viruses’ exonuclease activity. We examined these nucleotide analogues with regard to their ability to be incorporated by the RdRps in the polymerase reaction and then prevent further incorporation. While all 11 molecules tested displayed incorporation, 6 exhibited immediate termination of the polymerase reaction (Carbovir triphosphate, Ganciclovir triphosphate, Stavudine triphosphate, Entecavir triphosphate, 3’-O-methyl UTP and Biotin-16-dUTP), 2 showed delayed termination (Cidofovir diphosphate and 2’-O-methyl UTP), and 3 did not terminate the polymerase reaction (2’-fluoro-dUTP, 2’-amino-dUTP and Desthiobiotin-16-UTP). The coronavirus genomes encode an exonuclease that apparently requires a 2’ -OH group to excise mismatched bases at the 3’-terminus. In this study, all of the nucleoside triphosphate analogues we evaluated form Watson-Cricklike base pairs. All the nucleotide analogues which demonstrated termination either lack a 2’-OH, have a blocked 2’-OH, or show delayed termination. These nucleotides may thus have the potential to resist exonuclease activity, a property that we will investigate in the future. Furthermore, prodrugs of five of these nucleotide analogues (Brincidofovir/Cidofovir, Abacavir, Valganciclovir/Ganciclovir, Stavudine and Entecavir) are FDA approved for other viral infections, and their safety profile is well known. Thus, they can be evaluated rapidly as potential therapies for COVID-19.

Published

2020

10. Triphosphates of the Two Components in DESCOVY and TRUVADA are Inhibitors of the SARS-CoV-2 Polymerase

Author

Steffen Jockusch, James J. Russo, Xiaoxu Li, Robert N. Kirchdoerfer, Chuanjuan Tao, Minchen Chien, Jingyue Ju, Shiv Kumar, and Thomas K. Anderson

Subjects

Alovudine, biology, Sofosbuvir, business.industry, viruses, virus diseases, Emtricitabine, medicine.disease_cause, Virology, Tenofovir alafenamide, Virus, chemistry.chemical_compound, chemistry, RNA polymerase, biology.protein, medicine, business, Polymerase, medicine.drug, Coronavirus

Abstract

SARS-CoV-2, a member of the coronavirus family, is responsible for the current COVID-19 pandemic. We previously demonstrated that four nucleotide analogues (specifically, the active triphosphate forms of Sofosbuvir, Alovudine, AZT and Tenofovir alafenamide) inhibit the SARS-CoV-2 RNA-dependent RNA polymerase (RdRp). Tenofovir and emtricitabine are the two components in DESCOVY and TRUVADA, the two FDA-approved medications for use as pre-exposure prophylaxis (PrEP) to prevent HIV infection. This is a preventative method in which individuals who are HIV negative (but at high-risk of contracting the virus) take the combination drug daily to reduce the chance of becoming infected with HIV. PrEP can stop HIV from replicating and spreading throughout the body. We report here that the triphosphates of tenofovir and emtricitabine, the two components in DESCOVY and TRUVADA, act as terminators for the SARS-CoV-2 RdRp catalyzed reaction. These results provide a molecular basis to evaluate the potential of DESCOVY and TRUVADA as PrEP for COVID-19.

Published

2020

11. Nucleotide Analogues as Inhibitors of SARS-CoV Polymerase

Author

Steffen Jockusch, Chuanjuan Tao, Minchen Chien, Shiv Kumar, Sergey Kalachikov, James J. Russo, Xiaoxu Li, Robert N. Kirchdoerfer, Jingyue Ju, and Irina Morozova

Subjects

Antagonists & inhibitors, DNA polymerase, Hepatitis C virus, viruses, Pneumonia, Viral, RNA-dependent RNA polymerase, RM1-950, medicine.disease_cause, Antiviral Agents, Heterocyclic Compounds, 4 or More Rings, SARS‐CoV‐2, Betacoronavirus, chemistry.chemical_compound, COVID‐19, RNA polymerase, medicine, Humans, Thymine Nucleotides, General Pharmacology, Toxicology and Pharmaceutics, nucleotide analogue, skin and connective tissue diseases, Pandemics, Polymerase, Coronavirus, biology, SARS-CoV-2, fungi, COVID-19, SARS‐CoV, virus diseases, Original Articles, biochemical phenomena, metabolism, and nutrition, RNA-Dependent RNA Polymerase, Virology, Reverse transcriptase, body regions, RNA‐dependent RNA polymerase, Drug Combinations, Neurology, chemistry, biology.protein, Original Article, Carbamates, Therapeutics. Pharmacology, Sofosbuvir, Coronavirus Infections, Zidovudine, Dideoxynucleotides

Abstract

SARS‐CoV‐2, a member of the coronavirus family, has caused a global public health emergency. Based on our analysis of hepatitis C virus and coronavirus replication, and the molecular structures and activities of viral inhibitors, we previously reasoned that the FDA‐approved hepatitis C drug EPCLUSA (Sofosbuvir/Velpatasvir) should inhibit coronaviruses, including SARS‐CoV‐2. Here, using model polymerase extension experiments, we demonstrate that the active triphosphate form of Sofosbuvir is incorporated by low‐fidelity polymerases and SARS‐CoV RNA‐dependent RNA polymerase (RdRp), and blocks further incorporation by these polymerases; the active triphosphate form of Sofosbuvir is not incorporated by a host‐like high‐fidelity DNA polymerase. Using the same molecular insight, we selected 3’‐fluoro‐3’‐deoxythymidine triphosphate and 3’‐azido‐3’‐deoxythymidine triphosphate, which are the active forms of two other anti‐viral agents, Alovudine and AZT (an FDA‐approved HIV/AIDS drug) for evaluation as inhibitors of SARS‐CoV RdRp. We demonstrate the ability of two of these HIV reverse transcriptase inhibitors to be incorporated by SARS‐CoV RdRp where they also terminate further polymerase extension. Given the 98% amino acid similarity of the SARS‐CoV and SARS‐CoV‐2 RdRps, we expect these nucleotide analogues would also inhibit the SARS‐CoV‐2 polymerase. These results offer guidance to further modify these nucleotide analogues to generate more potent broad‐spectrum anti‐coronavirus agents., The triphosphate form of Sofosbuvir is incorporated by SARS‐CoV polymerase to terminate further primer extension, potentially preventing replication of the virus.

Published

2020

12. Nucleotide Analogues as Inhibitors of SARS-CoV-2 Polymerase

Author

Shiv Kumar, Chuanjuan Tao, Jingyue Ju, Robert N. Kirchdoerfer, Minchen Chien, Thomas K. Anderson, James J. Russo, Steffen Jockusch, and Xiaoxu Li

Subjects

Sofosbuvir, Hepatitis C virus, viruses, Pneumonia, Viral, Viral Nonstructural Proteins, medicine.disease_cause, Tenofovir alafenamide, Antiviral Agents, Article, chemistry.chemical_compound, Betacoronavirus, RNA polymerase, medicine, Humans, Pandemics, Polymerase, Coronavirus, Alovudine, biology, SARS-CoV-2, virus diseases, COVID-19, Hepatitis B, medicine.disease, RNA-Dependent RNA Polymerase, Virology, Dideoxynucleosides, chemistry, biology.protein, Coronavirus Infections, medicine.drug

Abstract

SARS-CoV-2 is responsible for the current COVID-19 pandemic. On the basis of our analysis of hepatitis C virus and coronavirus replication, and the molecular structures and activities of viral inhibitors, we previously demonstrated that three nucleotide analogues (the triphosphates of Sofosbuvir, Alovudine, and AZT) inhibit the SARS-CoV RNA-dependent RNA polymerase (RdRp). We also demonstrated that a library of additional nucleotide analogues terminate RNA synthesis catalyzed by the SARS-CoV-2 RdRp, a well-established drug target for COVID-19. Here, we used polymerase extension experiments to demonstrate that the active triphosphate form of Sofosbuvir (an FDA-approved hepatitis C drug) is incorporated by SARS-CoV-2 RdRp and blocks further incorporation. Using the molecular insight gained from the previous studies, we selected the active triphosphate forms of six other antiviral agents, Alovudine, Tenofovir alafenamide, AZT, Abacavir, Lamivudine, and Emtricitabine, for evaluation as inhibitors of the SARS-CoV-2 RdRp and demonstrated the ability of these viral polymerase inhibitors to be incorporated by SARS-CoV-2 RdRp, where they terminate further polymerase extension with varying efficiency. These results provide a molecular basis for inhibition of the SARS-CoV-2 RdRp by these nucleotide analogues. If sufficient efficacy of some of these FDA-approved drugs in inhibiting viral replication in cell culture is established, they may be explored as potential COVID-19 therapeutics.

Published

2020

13. Real-time single-molecule electronic DNA sequencing by synthesis using polymer-tagged nucleotides on a nanopore array

Author

James Pollard, Zengmin Li, Ashwini Bhat, Andrew Trans, Jennifer Hovis, Minchen Chien, Cleoma Arnold, Edward Shian Liu, Arek Bibillo, Randy Davis, John J. Kasianowicz, Mirko Palla, James J. Russo, Mintu Porel, Irina Morozova, Wenjing Guo, Jingyue Ju, Shundi Shi, Cynthia Cech, Shiv Kumar, Eric Takeshi Harada, Chuanjuan Tao, Carl W. Fuller, Alexander Yang, Michael Dorwart, Stefan Roever, Roger Chen, Anne Aguirre, George M. Church, Daniel Korenblum, P. Benjamin Stranges, and Sergey Kalachikov

Subjects

0301 basic medicine, Conductometry, Polymers, DNA polymerase, Nanotechnology, 010402 general chemistry, 01 natural sciences, DNA sequencing, Nanopores, 03 medical and health sciences, chemistry.chemical_compound, Computer Systems, Precision Medicine, Polymerase, Oligonucleotide Array Sequence Analysis, Multidisciplinary, Base Sequence, Staining and Labeling, biology, Nucleotides, Oligonucleotide, DNA, Equipment Design, Sequence Analysis, DNA, Biological Sciences, 0104 chemical sciences, Equipment Failure Analysis, Nanopore, 030104 developmental biology, chemistry, biology.protein, Biophysics, Nucleic acid, Primer (molecular biology)

Abstract

DNA sequencing by synthesis (SBS) offers a robust platform to decipher nucleic acid sequences. Recently, we reported a single-molecule nanopore-based SBS strategy that accurately distinguishes four bases by electronically detecting and differentiating four different polymer tags attached to the 5'-phosphate of the nucleotides during their incorporation into a growing DNA strand catalyzed by DNA polymerase. Further developing this approach, we report here the use of nucleotides tagged at the terminal phosphate with oligonucleotide-based polymers to perform nanopore SBS on an α-hemolysin nanopore array platform. We designed and synthesized several polymer-tagged nucleotides using tags that produce different electrical current blockade levels and verified they are active substrates for DNA polymerase. A highly processive DNA polymerase was conjugated to the nanopore, and the conjugates were complexed with primer/template DNA and inserted into lipid bilayers over individually addressable electrodes of the nanopore chip. When an incoming complementary-tagged nucleotide forms a tight ternary complex with the primer/template and polymerase, the tag enters the pore, and the current blockade level is measured. The levels displayed by the four nucleotides tagged with four different polymers captured in the nanopore in such ternary complexes were clearly distinguishable and sequence-specific, enabling continuous sequence determination during the polymerase reaction. Thus, real-time single-molecule electronic DNA sequencing data with single-base resolution were obtained. The use of these polymer-tagged nucleotides, combined with polymerase tethering to nanopores and multiplexed nanopore sensors, should lead to new high-throughput sequencing methods.

Published

2016

14. A library of nucleotide analogues terminate RNA synthesis catalyzed by polymerases of coronaviruses that cause SARS and COVID-19

Author

Chuanjuan Tao, Robert N. Kirchdoerfer, Thomas K. Anderson, Shiv Kumar, Minchen Chien, James J. Russo, Jingyue Ju, Steffen Jockusch, and Xiaoxu Li

Subjects

0301 basic medicine, Exonuclease, Guanine, Base pair, viruses, 030106 microbiology, Pneumonia, Viral, RNA-dependent RNA polymerase, Severe Acute Respiratory Syndrome, Tenofovir alafenamide, Antiviral Agents, Article, Nucleotide analogues, 03 medical and health sciences, chemistry.chemical_compound, Betacoronavirus, Virology, RNA polymerase, Valganciclovir, Prodrugs, Ganciclovir, Pandemics, Polymerase, Pharmacology, biology, SARS-CoV-2, Nucleotides, RNA, virus diseases, COVID-19, RNA-Dependent RNA Polymerase, Dideoxynucleosides, Stavudine, 030104 developmental biology, chemistry, Severe acute respiratory syndrome-related coronavirus, Nucleoside triphosphate, biology.protein, RNA, Viral, Coronavirus Infections, Cidofovir

Abstract

SARS-CoV-2, a member of the coronavirus family, is responsible for the current COVID-19 worldwide pandemic. We previously demonstrated that five nucleotide analogues inhibit the SARS-CoV-2 RNA-dependent RNA polymerase (RdRp), including the active triphosphate forms of Sofosbuvir, Alovudine, Zidovudine, Tenofovir alafenamide and Emtricitabine. We report here the evaluation of a library of nucleoside triphosphate analogues with a variety of structural and chemical features as inhibitors of the RdRps of SARS-CoV and SARS-CoV-2. These features include modifications on the sugar (2′ or 3′ modifications, carbocyclic, acyclic, or dideoxynucleotides) or on the base. The goal is to identify nucleotide analogues that not only terminate RNA synthesis catalyzed by these coronavirus RdRps, but also have the potential to resist the viruses' exonuclease activity. We examined these nucleotide analogues for their ability to be incorporated by the RdRps in the polymerase reaction and to prevent further incorporation. While all 11 molecules tested displayed incorporation, 6 exhibited immediate termination of the polymerase reaction (triphosphates of Carbovir, Ganciclovir, Stavudine and Entecavir; 3′-OMe-UTP and Biotin-16-dUTP), 2 showed delayed termination (Cidofovir diphosphate and 2′-OMe-UTP), and 3 did not terminate the polymerase reaction (2′-F-dUTP, 2′–NH2–dUTP and Desthiobiotin-16-UTP). The coronaviruses possess an exonuclease that apparently requires a 2′-OH at the 3′-terminus of the growing RNA strand for proofreading. In this study, all nucleoside triphosphate analogues evaluated form Watson-Crick-like base pairs. The nucleotide analogues demonstrating termination either lack a 2′-OH, have a blocked 2′-OH, or show delayed termination. Thus, these nucleotide analogues are of interest for further investigation to evaluate whether they can evade the viral exonuclease activity. Prodrugs of five of these nucleotide analogues (Cidofovir, Abacavir, Valganciclovir/Ganciclovir, Stavudine and Entecavir) are FDA-approved medications for treatment of other viral infections, and their safety profiles are well established. After demonstrating potency in inhibiting viral replication in cell culture, candidate molecules can be rapidly evaluated as potential therapies for COVID-19., Highlights • Cidofovir triphosphate is a delayed terminator for SARS-CoV-2 RNA polymerase. • Abacavir, Ganciclovir, and Stavudine triphosphates inhibit SARS-CoV-2 polymerase. • 2′-O-methylated UTP substantially terminates the SARS-CoV-2 polymerase reaction.

Published

2020

15. Design and characterization of a nanopore-coupled polymerase for single-molecule DNA sequencing by synthesis on an electrode array

Author

Shiv Kumar, James Pollard, Alexander Yang, Sergey Kalachikov, Mirko Palla, Minchen Chien, Mintu Porel, Jeff Nivala, Cleoma Arnold, Chuanjuan Tao, Roger Chen, Dmitriy Gremyachinskiy, Shundi Shi, Michael Dorwart, Randy Davis, Zengmin Li, Daniel Korenblum, Eric Takeshi Harada, Aman S. Aberra, P. Benjamin Stranges, James J. Russo, Arek Bibillo, Jingyue Ju, Carl W. Fuller, Stefan Roever, Anne Aguirre, Andrew Trans, George M. Church, Irina Morozova, and Ashwini Bhat

Subjects

DNA Replication, Models, Molecular, 0301 basic medicine, Polymers, Protein design, Porins, Nanotechnology, DNA-Directed DNA Polymerase, 02 engineering and technology, DNA sequencing, Nanopores, 03 medical and health sciences, A-DNA, Nucleotide, Electrodes, Polymerase, chemistry.chemical_classification, Multidisciplinary, biology, DNA synthesis, Nucleotides, High-Throughput Nucleotide Sequencing, Equipment Design, 021001 nanoscience & nanotechnology, Nanopore, 030104 developmental biology, PNAS Plus, chemistry, biology.protein, Biophysics, Nanopore sequencing, 0210 nano-technology

Abstract

Scalable, high-throughput DNA sequencing is a prerequisite for precision medicine and biomedical research. Recently, we presented a nanopore-based sequencing-by-synthesis (Nanopore-SBS) approach, which used a set of nucleotides with polymer tags that allow discrimination of the nucleotides in a biological nanopore. Here, we designed and covalently coupled a DNA polymerase to an α-hemolysin (αHL) heptamer using the SpyCatcher/SpyTag conjugation approach. These porin-polymerase conjugates were inserted into lipid bilayers on a complementary metal oxide semiconductor (CMOS)-based electrode array for high-throughput electrical recording of DNA synthesis. The designed nanopore construct successfully detected the capture of tagged nucleotides complementary to a DNA base on a provided template. We measured over 200 tagged-nucleotide signals for each of the four bases and developed a classification method to uniquely distinguish them from each other and background signals. The probability of falsely identifying a background event as a true capture event was less than 1.2%. In the presence of all four tagged nucleotides, we observed sequential additions in real time during polymerase-catalyzed DNA synthesis. Single-polymerase coupling to a nanopore, in combination with the Nanopore-SBS approach, can provide the foundation for a low-cost, single-molecule, electronic DNA-sequencing platform.

Published

2016

16. PEG-Labeled Nucleotides and Nanopore Detection for Single Molecule DNA Sequencing by Synthesis

Author

Chuanjuan Tao, Minchen Chien, Joseph E. Reiner, Shiv Kumar, Zengmin Li, John J. Kasianowicz, Arvind Balijepalli, James J. Russo, Joseph W. F. Robertson, Brittney Hellner, and Jingyue Ju

Subjects

02 engineering and technology, Polymerase Chain Reaction, DNA sequencing, Article, law.invention, Polyethylene Glycols, 03 medical and health sciences, chemistry.chemical_compound, Nanopores, Electricity, law, Coumarins, Molecule, Nucleotide, Polymerase chain reaction, Polymerase, 030304 developmental biology, Fluorescent Dyes, chemistry.chemical_classification, 0303 health sciences, Multidisciplinary, biology, Staining and Labeling, Chemistry, Nucleotides, Deoxyguanine Nucleotides, DNA, Electrochemical Techniques, Sequence Analysis, DNA, 021001 nanoscience & nanotechnology, Molecular Weight, Nanopore, Biochemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, biology.protein, Biophysics, 0210 nano-technology, Single molecule real time sequencing

Abstract

We describe a novel single molecule nanopore-based sequencing by synthesis (Nano-SBS) strategy that can accurately distinguish four bases by detecting 4 different sized tags released from 5'-phosphate-modified nucleotides. The basic principle is as follows. As each nucleotide is incorporated into the growing DNA strand during the polymerase reaction, its tag is released and enters a nanopore in release order. This produces a unique ionic current blockade signature due to the tag's distinct chemical structure, thereby determining DNA sequence electronically at single molecule level with single base resolution. As proof of principle, we attached four different length PEG-coumarin tags to the terminal phosphate of 2'-deoxyguanosine-5'-tetraphosphate. We demonstrate efficient, accurate incorporation of the nucleotide analogs during the polymerase reaction, and excellent discrimination among the four tags based on nanopore ionic currents. This approach coupled with polymerase attached to the nanopores in an array format should yield a single-molecule electronic Nano-SBS platform.

Published

2012

17. Design and characterization of a nanopore-coupled polymerase for single-molecule DNA sequencing by synthesis on an electrode array.

Author

Stranges, P. Benjamin, Pallaa, Mirkó, Kalachikov, Sergey, Nivala, Jeff, Dorwart, Michael, Trans, Andrew, Kumar, Shiv, Porel, Mintu, Minchen Chien, Chuanjuan Tao, Morozova, Irina, Zengmin Li, Shundi Shi, Aberrae, Aman, Arnold, Cleoma, Yang, Alexander, Aguirre, Anne, Harada, Eric T., Korenblum, Daniel, and Pollard, James

Subjects

POLYMERASES, NANOPORES, NUCLEOTIDE sequencing, MEDICAL research, NUCLEOTIDES

Abstract

Scalable, high-throughput DNA sequencing is a prerequisite for precision medicine and biomedical research. Recently, we presented a nanopore-based sequencing-by-synthesis (Nanopore-SBS) approach, which used a set of nucleotides with polymer tags that allow discrimination of the nucleotides in a biological nanopore. Here, we designed and covalently coupled a DNA polymerase to an α-hemolysin (αHL) heptamer using the SpyCatcher/SpyTag conjugation approach. These porin-polymerase conjugates were inserted into lipid bilayers on a complementary metal oxide semiconductor (CMOS)-based electrode array for high-throughput electrical recording of DNA synthesis. The designed nanopore construct successfully detected the capture of tagged nucleotides complementary to a DNA base on a provided template. We measured over 200 tagged-nucleotide signals for each of the four bases and developed a classification method to uniquely distinguish them from each other and background signals. The probability of falsely identifying a background event as a true capture event was less than 1.2%. In the presence of all four tagged nucleotides, we observed sequential additions in real time during polymerase-catalyzed DNA synthesis. Single-polymerase coupling to a nanopore, in combination with the Nanopore-SBS approach, can provide the foundation for a low-cost, single-molecule, electronic DNA-sequencing platform. [ABSTRACT FROM AUTHOR]

Published

2016

18. Real-time single-molecule electronic DNA sequencing by synthesis using polymer-tagged nucleotides on a nanopore array.

Author

Fuller, Carl W., Kumar, Shiv, Porel, Mintu, Minchen Chien, Bibillo, Arek, Stranges, P. Benjamin, Dorwart, Michael, Chuanjuan Tao, Zengmin Li, Wenjing Guo, Shundi Shi, Korenblum, Daniel, Trans, Andrew, Aguirre, Anne, Liu, Edward, Harada, Eric T., Pollard, James, Bhat, Ashwini, Cech, Cynthia, and Yang, Alexander

Subjects

NUCLEOTIDE sequencing, DNA polymerases, NUCLEOTIDES, NANOPORES, HEMOLYSIS & hemolysins

Abstract

DNA sequencing by synthesis (SBS) offers a robust platform to decipher nucleic acid sequences. Recently, we reported a singlemolecule nanopore-based SBS strategy that accurately distinguishes four bases by electronically detecting and differentiating four different polymer tags attached to the 5'-phosphate of the nucleotides during their incorporation into a growing DNA strand catalyzed by DNA polymerase. Further developing this approach, we report here the use of nucleotides tagged at the terminal phosphate with oligonucleotide-based polymers to perform nanopore SBS on an α-hemolysin nanopore array platform. We designed and synthesized several polymer-tagged nucleotides using tags that produce different electrical current blockade levels and verified they are active substrates for DNA polymerase. A highly processive DNA polymerase was conjugated to the nanopore, and the conjugates were complexed with primer/template DNA and inserted into lipid bilayers over individually addressable electrodes of the nanopore chip. When an incoming complementary-tagged nucleotide forms a tight ternary complex with the primer/template and polymerase, the tag enters the pore, and the current blockade level is measured. The levels displayed by the four nucleotides tagged with four different polymers captured in the nanopore in such ternary complexes were clearly distinguishable and sequence-specific, enabling continuous sequence determination during the polymerase reaction. Thus, real-time single-molecule electronic DNA sequencing data with single-base resolution were obtained. The use of these polymer-tagged nucleotides, combined with polymerase tethering to nanopores and multiplexed nanopore sensors, should lead to new high-throughput sequencing methods. [ABSTRACT FROM AUTHOR]

Published

2016

19. Searching for the cosmion by scattering in Si detectors

Author

D. Yvon, Richard H. Pehl, A. Da Silva, A. R. Smith, E. Lesquoy, M. Spiro, J. Rich, B. Magnusson, D. A. Landis, Fred S. Goulding, Bernard Sadoulet, C. A. Cork, Norman W. Madden, Chuanjuan Tao, S. Zylberajch, Michael S. Witherell, G. Gerbier, and D. O. Caldwell

Subjects

Physics, Nuclear physics, Particle scattering, Particle physics, Scattering, Ionization, Dark matter, Energy spectrum, General Physics and Astronomy, Elementary particle, Cosmology

Abstract

Une nouvelle particule, le cosmion (particule massive a interaction faible), a ete proposee pour resoudre le probleme de la matiere sombre dans l'univers, et pour expliquer le deficit ν solaire par refroidissement du noyau solaire pour reduire la production 8 B ν. Les mesures ont ete effectuees dans les detecteurs a ionisation Si jusqu'aux energies inferieures de 1.1 keV

Published

1990

20. Dark matter detection with hydrogen proportional counters

Author

J. Rich, G. Gerbier, M. Spiro, and Chuanjuan Tao

Subjects

Physics, Nuclear and High Energy Physics, Hydrogen, chemistry, Mixed dark matter, Dark matter, chemistry.chemical_element, Astrophysics, Atomic and Molecular Physics, and Optics

Published

1990